XAF1 通过组装 ZNF313 介导的破坏复合物来拮抗 TRIM28 的活性,从而抑制肿瘤的恶性发展。

IF 6.3 Q1 BIOCHEMISTRY & MOLECULAR BIOLOGY Molecular biomedicine Pub Date : 2024-11-13 DOI:10.1186/s43556-024-00224-9
Seung-Hun Jang, Hwi-Wan Choi, Jieun Ahn, Sungchan Jang, Ji-Hye Yoon, Min-Goo Lee, Sung-Gil Chi
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引用次数: 0

摘要

X连锁凋亡相关因子1抑制因子(XAF1)是一种应激诱导的促凋亡蛋白,在多种人类癌症中普遍失活。然而,其抑制肿瘤功能的分子基础在很大程度上仍未定性。在这里,我们报告了 XAF1 通过锌指蛋白 313(ZNF313)诱导的泛素化和蛋白酶体降解,拮抗了含三方基序 28(TRIM28)泛素 E3 连接酶的致癌活性。XAF1在TRIM28+/+与XAF1-/-肿瘤细胞中发挥更强的促进凋亡作用,并以高度依赖TRIM28的方式抑制肿瘤细胞的生长、迁移、侵袭、上皮细胞向间质转化以及异种移植肿瘤的生长。从机理上讲,XAF1 通过 ZF6 和 ZF7 结构域分别与 TRIM28 和 ZNF313 的 RING 结构域直接相互作用,从而促进 ZNF313 与 TRIM28 的相互作用和泛素化。缺乏 ZF6 或 ZF7 结构域的突变体 XAF1 没有促进 TRIM28 泛素化的活性。通过破坏 TRIM28 的稳定性,XAF1 阻断了 TRIM28 驱动的 p53 和 RLIM 泛素化、p53-HDAC1 相互作用以及 TWIST1 稳定。耐人寻味的是,TRIM28 通过与 K48 链接的多泛素化和蛋白酶体降解来破坏 XAF1 的稳定性,从而保护肿瘤细胞免受凋亡压力,这表明它是 XAF1 的内在拮抗剂,也表明 XAF1 和 TRIM28 之间存在拮抗作用。在癌细胞系和肿瘤组织中,XAF1的表达与TRIM28的表达成反比,并且与TRIM28高表达患者的存活率相比,与TRIM28低表达患者的存活率关系更为密切。总之,这项研究发现了 XAF1 抑制肿瘤恶性程度的新机制,以及 XAF1-TRIM28 在应激反应中的重要作用,揭示了其在肿瘤发生过程中发生改变的机理。
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XAF1 antagonizes TRIM28 activity through the assembly of a ZNF313-mediated destruction complex to suppress tumor malignancy.

X-linked inhibitor of apoptosis-associated factor 1 (XAF1) is a stress-inducible pro-apoptotic protein that is commonly inactivated in multiple human cancers. Nevertheless, the molecular basis for its tumor suppression function remains largely uncharacterized. Here we report that XAF1 antagonizes the oncogenic activity of tripartite motif containing 28 (TRIM28) ubiquitin E3 ligase through zinc finger protein 313 (ZNF313)-induced ubiquitination and proteasomal degradation. XAF1 exerts apoptosis-promoting effect more strongly in TRIM28+/+ versus XAF1-/- tumor cells and suppresses tumor cell growth, migration, invasion, and epithelial-to-mesenchymal transition and xenograft tumor growth in a highly TRIM28-dependent fashion. Mechanistically, XAF1 interacts directly with the RING domains of TRIM28 and ZNF313 through the ZF6 and ZF7 domain, respectively, thereby facilitating ZNF313 interaction with and ubiquitination of TRIM28. A mutant XAF1 lacking either ZF6 or ZF7 domain exhibits no activity to promote TRIM28 ubiquitination. By destabilizing TRIM28, XAF1 blocks TRIM28-driven ubiquitination of p53 and RLIM, p53-HDAC1 interaction, and TWIST1 stabilization. Intriguingly, TRIM28 destabilizes XAF1 through K48-linked polyubiquitination and proteasomal degradation to protect tumor cells from apoptotic stress, indicating its role as an intrinsic antagonist against XAF1 and the antagonistic interplay of XAF1 and TRIM28. XAF1 expression is inversely correlated with TRIM28 expression in cancer cell lines and tumor tissues and more tightly associated with the survival of TRIM28-high versus TRIM28-low patients. Together, this study uncovers a novel mechanism by which XAF1 suppresses tumor malignancy and an important role for XAF1-TRIM28 interplay in governing stress response, illuminating the mechanistic consequence of its alteration during tumorigenic process.

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